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Peer-reviewed veterinary case report

Leishmania amazonensis vaccine triggers protective immune response

By Petitdidier, Elodie et al.·Published in PLoS neglected tropical diseases·2016·IRD, France·View original on PubMed

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Original publication title: Recombinant Forms of Leishmania amazonensis Excreted/Secreted Promastigote Surface Antigen (PSA) Induce Protective Immune Responses in Dogs.

Species:
dog

Plain-English summary

A group of Beagle dogs was vaccinated to protect against leishmaniasis, a disease caused by parasites. The dogs received three doses of a new vaccine made from a specific protein (LaPSA) found in the parasite, along with an immune-boosting agent. Six months later, about 79% of the vaccinated dogs showed no signs of the parasite in their bone marrow, and those that were infected had much lower levels of the parasite compared to unvaccinated dogs. The vaccine also triggered a strong immune response, suggesting it could be a promising option for preventing this disease in dogs.

People also search for: dog leishmaniasis vaccine · Beagle leishmaniasis prevention · leishmaniasis symptoms in dogs

Abstract

Preventive vaccination is a highly promising strategy for interrupting leishmaniasis transmission that can, additionally, contribute to elimination. A vaccine formulation based on naturally excreted secreted (ES) antigens was prepared from L. infantum promastigote culture supernatant. This vaccine achieved successful results in Phase III trials and was licensed and marketed as CaniLeish. We recently showed that newly identified ES promastigote surface antigen (PSA), from both viable promastigotes and axenically-grown amastigotes, represented the major constituent and the highly immunogenic antigen of L. infantum and L. amazonensis ES products. We report here that three immunizations with either the recombinant ES LaPSA-38S (rPSA) or its carboxy terminal part LaPSA-12S (Cter-rPSA), combined with QA-21 as adjuvant, confer high levels of protection in naive L. infantum-infected Beagle dogs, as checked by bone marrow parasite absence in respectively 78.8% and 80% of vaccinated dogs at 6 months post-challenge. The parasite burden in infected vaccinated dogs was significantly reduced compared to placebo group, as measured by q-PCR. Moreover, our results reveal humoral and cellular immune response clear-cut differences between vaccinated and control dogs. An early increase in specific IgG2 antibodies was observed in rPSA/QA-21- and Cter-rPSA/QA-21-immunized dogs only. They were found functionally active in vitro and were highly correlated with vaccine protection. In vaccinated protected dogs, IFN-γ and NO productions, as well as anti-leishmanial macrophage activity, were increased. These data strongly suggest that ES PSA or its carboxy-terminal part, in recombinant forms, induce protection in a canine model of zoonotic visceral leishmaniasis by inducing a Th1-dominant immune response and an appropriate specific antibody response. These data suggest that they could be considered as important active components in vaccine candidates.

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Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/27223609/